Early life exposure to nicotine modifies lung gene response after elastase-induced emphysema
Autor: | Blaskovic, Sanja, Donati, Yves, Ruchonnet-Metrailler, Isabelle, Avila, Yannick, Schittny, Dominik, Schlep��tz, Christian Matthias, Schittny, Johannes, Barazzone-Argiroffo, Constance |
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Rok vydání: | 2022 |
Předmět: |
Emphysema
Nicotine ddc:618 Pancreatic Elastase Histocompatibility Antigens Class I H-2 Antigens 610 Medicine & health ddc:616.07 Mice Inbred C57BL Disease Models Animal Mice Life Expectancy Gene Expression Regulation Pulmonary Emphysema Animals RNA Lung development Bronchoalveolar Lavage Fluid Cells Cultured |
Zdroj: | Respiratory research, Vol. 23, No 1 (2022) P. 44 Blaskovic, Sanja; Donati, Yves; Ruchonnet-Metrailler, Isabelle; Avila, Yannick; Schittny, Dominik; Schlepütz, Christian Matthias; Schittny, Johannes; Barazzone-Argiroffo, Constance (2022). Early life exposure to nicotine modifies lung gene response after elastase-induced emphysema. Respiratory research, 23(1), p. 44. BioMed Central 10.1186/s12931-022-01956-4 |
ISSN: | 1465-9921 |
DOI: | 10.48350/166597 |
Popis: | Background: Chronic obstructive pulmonary disease (COPD) is among the top 5 causes of mortality in the world and can develop as a consequence of genetic and/or environmental factors. Current efforts are focused on identifying early life insults and how these contribute to COPD development. In line with this, our study focuses on the influence of early life nicotine exposure and its potential impact on (a) lung pulmonary functions, and (b) elastase-induced emphysema in adulthood.Methods: To address this hypothesis, we developed a model of 2 hits, delivered at different time points: mouse pups were first exposed to nicotine/placebo in utero and during lactation, and then subsequently received elastase/placebo at the age of 11 weeks. The effect of nicotine pretreatment and elastase instillation was assessed by (a) measurement of pulmonary function at post-elastase day (ped) 21, and (b) transcriptomic profiling at ped3 and 21, and complementary protein determination. Statistical significance was determined by 3- and 2-way ANOVA for pulmonary functions, and RNAseq results were analyzed using the R project.Results: We did not observe any impact of nicotine pre- and early post-natal exposure compared to control samples on lung pulmonary functions in adulthood, as measured by FLEXIVENT technology. After elastase instillation, substantial lung damage was detected by x-ray tomography and was accompanied by loss in body weight at ped3 as well as an increase in cell numbers, inflammatory markers in BAL and lung volume at ped21. Lung functions showed a decrease in elastance and an increase in deep inflation volume and pressure volume (pv) loop area in animals with emphysema at ped21. Nicotine had no effect on elastance and deep inflation volume, but did affect the pv loop area in animals with emphysema at ped21. Extensive transcriptomic changes were induced by elastase at ped3 both in the nicotine-pretreated and the control samples, with several pathways common to both groups, such as for cell cycle, DNA adhesion and DNA damage. Nicotine pretreatment affected the number of lymphocytes present in BAL after elastase instillation and some of the complement pathway related proteins, arguing for a slight modification of the immune response, as well as changes related to general body metabolism. The majority of elastase-induced transcriptomic changes detected at ped3 had disappeared at ped21. In addition, transcriptomic profiling singled out a common gene pool that was independently activated by nicotine and elastase.Conclusions: Our study reports a broad spectrum of transient transcriptomic changes in mouse emphysema and identifies nicotine as influencing the emphysema-associated immune system response. |
Databáze: | OpenAIRE |
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